EMA/258177/2014 Summary of the risk management plan (RMP) for Laventair (umeclidinium bromide and vilanterol) This is a summary of the risk management plan (RMP) for Laventair, which details the measures to be taken in order to ensure that Laventair is used as safely as possible. For more information on RMP summaries, see here. This RMP summary should be read in conjunction with the EPAR summary and the product information for Laventair, which can be found on Laventair s EPAR page. Overview of disease epidemiology Chronic obstructive pulmonary disease (COPD) is a long-term disease in which the airways and air sacs inside the lungs become damaged or blocked, leading to difficulty breathing. Symptoms of COPD usually develop over a number of years and can include breathlessness (especially after physical activity), persistent cough sometimes with mucus, wheezing, and frequent chest infections. The main cause of COPD is smoking. The disease is aggravated by bacterial and viral chest infections which cause exacerbations (flare-ups). Both exacerbations and chest infections can require admission to hospital and in some cases can lead to death. It is estimated that there are around 210 million people with COPD worldwide. Males are more often affected than females and Europeans are more often affected than Asians and particularly more than Africans. Generally, with increasing age, more people suffer from COPD. Less than 6% of people between the ages of 25-44 years suffer from mild and moderate COPD, while, more than 40% of people in the age group of 75 years and older suffer from mild and moderate COPD. Summary of treatment benefits Laventair contains two active substances. One active substance, umeclidinium bromide, is a longacting muscarinic receptor antagonist (LAMA) and the other, vilanterol, is a long-acting beta2- adrenoceptor agonist (LABA). Both medicines work in a complementary way to help open up the airways. Both classes of medicines (LAMA and LABA) are frequently used to treat the symptoms of COPD. Laventair is indicated as a maintenance bronchodilator treatment to relieve symptoms in adult patients with chronic obstructive pulmonary disease (COPD). Laventair was studied in 5 main studies of 6 months duration which involved 5,618 patients. These patients received either umeclidinium bromide and vilanterol, umeclidinium bromide alone, vialnterol alone, tiotropium ( another LAMA) or placebo (dummy treatment). The results showed an improvement in breathing (as measured by spirometry) for Laventair when compared with its individual components, umeclidinium bromide and vilanterol. Compared with placebo there was also a clear improvement in breathlessness associated with COPD in addition to an improvement in breathing. Laventair also improved breathing and provided a similar effect on breathlessness compared with tiotropium. Taken together, the results from all the studies support the Page 1/6
use of Laventair as a once-daily bronchodilator treatment to relieve symptoms in adult patients with COPD. Unknowns relating to treatment benefits The majority of subjects were white (80-89%), majority were male (63-69%) and subjects had a mean age of 62-64 years, across all treatment groups. There is no evidence to suggest that results would be different in non-white subjects. Summary of safety concerns Important identified risks None identified. Important potential risks Risk Problems affecting the heart and the blood vessels in the brain. (Cardiovascular and cerebrovascular disorders) Vilanterol is a LABA and umeclidinium bromide is a LAMA. It is known that other LAMAs and LABAs have been associated with effects on the heart such as irregular heart beat (including atrial fibrillation and tachycardia) and cerebrovascular events (stroke, transient ischaemic attack and central nervous system haemorrhage). Laventair should be used with caution in patients with severe heart problems. Increase in hospitalisation and death due to asthma, in patients with asthma. (Asthma-related intubations and deaths) One of the medicines contained in Laventair is a long acting beta2-adrenoceptor agonist (LABA). In studies in patients with asthma using a LABA alone, a higher number of patients with asthma were hospitalised, and died from their asthma. Laventair has not been studied in patients with asthma and should therefore not be used in asthma. Increased hospitalisation and death have not been seen in patients with COPD, even if they had previously been diagnosed with asthma. Temporary narrowing of the airways (paradoxical bronchospasm) which occurs suddenly leading to difficulties in breathing or wheezing. (Paradoxical bronchospasm) In studies with Laventair, paradoxical bronchospasm- which can be life-threatening has not been observed. However, it has been observed with other inhalation therapy where it occurred straight after taking the medicine. If patients develop any of these symptoms, the use of Laventair should be stopped and medical help should be sought immediately. Narrow angle glaucoma (a type of high pressure One of the active substances contained in Page 2/6
Risk in the eye) Laventair, umeclidinium, is a LAMA. These types of medicines have been reported to cause a rare type of glaucoma called narrow angle glaucoma. The medicine should be used with caution in patients with increased pressure in the eye (or narrow-angle glaucoma). If patients suffer from changes in vision or eye pain, they should stop taking the medicine and tell their doctor immediately. Sudden inability to pass urine (Urinary retention) LAMAs have been reported to cause a sudden inability to pass urine (urinary retention). Some elderly male patients who have other medical conditions, such as an enlarged prostate may be more prone to urinary retention. It is important for COPD to be well treated, so some patients with these conditions may receive Laventair following medical advice. Missing information Risk Safety in patients who are pregnant or who are currently breast feeding For Laventair, no clinical data on exposure during pregnancy are available. During pregnancy, Laventair should be used with caution. In patients with COPD who become pregnant, it is important that COPD is controlled, so some patients may receive Laventair following medical advice. It is not known whether Laventair passes into human breast milk and it should therefore be used with caution in breastfeeding women. Off-label use in patients with Asthma (this does not include patients with COPD who have either previously had asthma, or who have COPD and asthma) Laventair is not to be used in asthma. Studies with Laventair have not been done in patients with asthma, so it is not known if Laventair is of benefit in these patients. Safety in patients who have used the medicine long-term LAMAs and LABAs have been used successfully in the long-term treatment of COPD (beyond one year). Laventair has been studied for periods of up to one year. Despite this limited information, there is no indication that Laventair is less safe Page 3/6
Risk when used long term. Use in patients with severe liver problems Patients who have severe liver problems were not included in the studies. Therefore, the safety of Laventair in these patients is unknown. It is important for COPD to be well treated, so some patients with severe liver problems may receive Laventair following medical advice. Interaction with other medicines Laventair has been tested to see if it interacts with other medicines. Some additional laboratory studies have been requested. As some medicines may affect how Laventair works, patients should tell their doctor or pharmacist if they are taking, have recently taken or might take any other medicines. Summary of risk minimisation measures by safety concern All medicines have a summary of product characteristics (SmPC) which provides physicians, pharmacists and other healthcare professionals with details on how to use the medicine, and also describes the risks and recommendations for minimising them. Information for patients is available in lay language in the package leaflet. The measures listed in these documents are known as routine risk minimisation measures. The SmPC and the package leaflet are part of the medicine s product information. The product information for Laventair can be found on Laventair s EPAR page. This medicine has no additional risk minimisation measures. Planned post-authorisation development plan List of studies in post-authorisation development plan Study/activity (including study number) Objectives Safety concerns /efficacy issue addressed Status Planned date for submission of (interim and) final results Study 201038 Post- Authorisation Safety Observational Cohort Study to Quantify the Incidence and Comparative Safety To quantify the incidence of cardiovascular and cerebrovascular events of interest after the start of exposure to umeclidinium bromide (UMEC)/vilanterol (VI) in Cardio- and Cerebrovascular Disorders Lower respiratory tract infections (including pneumonia) Planned Final report: Q3 2024 Page 4/6
Study/activity (including study number) Objectives Safety concerns /efficacy issue addressed Status Planned date for submission of (interim and) final results of Selected Cardiovascular and Cerebrovascular Events in COPD patients using Inhaled UMEC/VI or Inhaled UMEC versus Tiotropium Handihaler (Study 201038). the licensed indication, in the post marketing setting, specifically in the COPD patients managed in primary care in multiple European countries and compare with the incidence of cardiovascular and cerebrovascular events of interest after the start of exposure to tiotropium (Handihaler) over 24 months follow-up. Safety in long-term use Study WWE117397 (formerly WEUSKOP6679): Post-authorisation Safety Electronic Medical Records Database Cohort Study of New Users of Inhaled UMEC/VI or New Users of Inhaled UMEC in the Primary Care Setting: UK EMR Distributed Network Study. Primary: Drug utilisation review of new users of UMEC/VI or new users of UMEC compared to COPD patients initiating longacting bronchodilators. Secondary: Quantify the disease burden of COPD and estimate the incidence of cardiovascular events of interest among new users of UMEC/VI, new users of UMEC and a comparator (selected from new long-acting bronchodilator users) among those with no ongoing management for the events of interest at observation start. Cardio- and Cerebrovascular Disorders Lower respiratory tract infections (including pneumonia) Off-label use Planned Final report: Q4 2019 Regulatory review of the UMEC/VI submission has highlighted additional in vitro drug interaction investigations which should be Additional investigations to provide information to: Address the binding of UMEC to microsomes and recalculation of I/Ki in the gut Additional in vitro investigations of Drug Interactions Planned Final report: Q1 2015 Page 5/6
Study/activity (including study number) Objectives Safety concerns /efficacy issue addressed Status Planned date for submission of (interim and) final results completed. based on free drug concentrations provide data for VI as a substrate of OATP1B1 and 1B3 provide data for UMEC as a substrate for BCRP and BSEP provide further clarification for the lack of effect of UMEC in CYP 2D6 poor metaboliser, possibly through studies in microsomes and hepatocytes provide data for UMEC as a substrate of OATP1B1 and 1B3 Studies which are a condition of the marketing authorisation Study 201038 is a condition of the market authorisation. Summary of changes to the risk management plan over time Not applicable. This summary was last updated in 05-2014. Page 6/6